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Vol. 27, Issue 10, 1123-1127, October 1999
Wadsworth Center, New York State Department of Health, Albany, New
York
Cytochrome P-450 (CYP) 2J4 is a member of the
recently identified CYP2J subfamily-part of the CYP superfamily-and
is primarily expressed in rat small intestinal epithelium
(enterocytes). Studies to determine small intestinal CYP2J4
inducibility by prototypic CYP inducers have been undertaken.
Immunoblot analysis of enterocyte microsomes from rats treated with
-naphthoflavone, dexamethasone, or phenobarbital revealed unchanged,
diminished, or slightly increased levels of CYP2J4 protein,
respectively, relative to vehicle-treated rats, whereas rats treated
with pyrazole (200 mg/kg) had 3- to 4-fold increased levels of CYP2J4.
Pyrazole administration also increased CYP2J4 metabolic activity, as
probed by retinoic acid formation from retinal, approximately 3-fold,
and the activity was inhibited by 90% by a polyclonal anti-CYP2J4
antibody. CYP2J4 mRNA levels were increased 2.5-fold by pyrazole
administration. The route of pyrazole administration-oral or i.p.-did
not affect the extent or time course of intestinal CYP2J4 induction.
However, at >300 mg/kg pyrazole, oral administration produced higher
levels of CYP2J4 activity than i.p. administration. Pyrazole also
produced increased hepatic and olfactory mucosal levels of CYP2J4. We
speculate, based on our data and on published mechanisms of pyrazole
induction, that pyrazole induces rat intestinal CYP2J4 by stabilization
of mRNA primarily, and by stabilization of protein to a lesser extent. This study documents for the first time the induction of a CYP2J subfamily member by a xenobiotic and provides the basis for a mechanism
by which xenobiotics could modulate biological processes.
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